Early growth response 1 and fatty acid synthase expression is altered in tumor adjacent prostate tissue and indicates field cancerization

Jones, Aaron P.; Trujillo, Kristina A.; Phillips, Genevieve K; Fleet, Trisha; Murton, Jaclyn K.; Severns, Virginia; Shah, Satyan K.; Davis, Michael S.; Smith, Anthony Y.; Griffith, Jeffrey K.; Fischer, Eva; Bisoffi, Marco

doi:10.1002/pros.22465

Cited by 14 publications

(40 citation statements)

References 36 publications

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“…In contrast, detection of molecular cancer field effects that are not microscopically visible to the pathologist could increase sensitivity for occult PC and ensure early diagnosis of potentially aggressive tumours. PC associated field effects have previously been detected at various molecular levels, including RNA3031, protein3334 and DNA (mutations)32. Here, we focused specifically on epigenetic field effects since aberrant DNA methylation has been found to be an early and highly recurrent event in PC16.…”

Section: Discussionmentioning

confidence: 99%

“…So far, field effects in relation to PC have been reported at various molecular levels, including RNA3031, DNA32, protein3334, and DNA methylation35363738, where the latter seems particularly promising. Indeed, a commercial test (ConfirmMDx for Prostate Cancer, MDx Health), based on APC (Adenomatous Polyposis Coli), GSTP1 , and RASSF1 (Ras Association (RalGDS/AF-6) Domain Family Member 1) hypermethylation in cancer-negative biopsies, offers a negative predictive value of 90%39.…”

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confidence: 99%

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Heterogeneous patterns of DNA methylation-based field effects in histologically normal prostate tissue from cancer patients

Moller

Strand

Mundbjerg

et al. 2017

Sci Rep

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Prostate cancer (PC) diagnosis is based on histological evaluation of prostate needle biopsies, which have high false negative rates. Here, we investigated if cancer-associated epigenetic field effects in histologically normal prostate tissue may be used to increase sensitivity for PC. We focused on nine genes (AOX1, CCDC181 (C1orf114), GABRE, GAS6, HAPLN3, KLF8, MOB3B, SLC18A2, and GSTP1) known to be hypermethylated in PC. Using quantitative methylation-specific PCR, we analysed 66 malignant and 134 non-malignant tissue samples from 107 patients, who underwent ultrasound-guided prostate biopsy (67 patients had at least one cancer-positive biopsy, 40 had exclusively cancer-negative biopsies). Hypermethylation was detectable for all genes in malignant needle biopsy samples (AUC: 0.80 to 0.98), confirming previous findings in prostatectomy specimens. Furthermore, we identified a four-gene methylation signature (AOX1xGSTP1xHAPLN3xSLC18A2) that distinguished histologically non-malignant biopsies from patients with vs. without PC in other biopsies (AUC = 0.65; sensitivity = 30.8%; specificity = 100%). This signature was validated in an independent patient set (59 PC, 36 adjacent non-malignant, and 9 normal prostate tissue samples) analysed on Illumina 450 K methylation arrays (AUC = 0.70; sensitivity = 40.6%; specificity = 100%). Our results suggest that a novel four-gene signature may be used to increase sensitivity for PC diagnosis through detection of epigenetic field effects in histologically non-malignant prostate tissue samples.

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Section: Discussionmentioning

confidence: 99%

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confidence: 99%

Heterogeneous patterns of DNA methylation-based field effects in histologically normal prostate tissue from cancer patients

Moller

Strand

Mundbjerg

et al. 2017

Sci Rep

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“…Quantitative immunofluorescence was performed as described in our previous work [ 12 ]. Briefly, paraffin-embedded prostate tissue sections were deparaffinized with xylene and rehydrated with decreasing concentrations of ethanol.…”

Section: Methodsmentioning

confidence: 99%

“…Accordingly, a number of genetic, epigenetic, and biochemical alterations in structurally intact cells of both epithelial and stromal origin that reside in histologically normal tissues adjacent to prostate adenocarcinomas (“field cancerized” tissues) have been recently identified by us and others and postulated to be of value as clinical indicators of disease (reviewed in [ 7 – 10 ]). We have previously identified, among others, the key transcription factor early growth response 1 (EGR-1) and the lipogenic enzyme fatty acid synthase (FAS) as distinct markers of prostate field cancerization [ 11 , 12 ]. Of note, growth factors and cytokines have not been previously described in the context of field cancerization.…”

Section: Introductionmentioning

confidence: 99%

Prostate Field Cancerization: Deregulated Expression of Macrophage Inhibitory Cytokine 1 (MIC-1) and Platelet Derived Growth Factor A (PDGF-A) in Tumor Adjacent Tissue

et al. 2015

Self Cite

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Prostate field cancerization denotes molecular alterations in histologically normal tissues adjacent to tumors. Such alterations include deregulated protein expression, as we have previously shown for the key transcription factor early growth response 1 (EGR-1) and the lipogenic enzyme fatty acid synthase (FAS). Here we add the two secreted factors macrophage inhibitory cytokine 1 (MIC-1) and platelet derived growth factor A (PDGF-A) to the growing list of protein markers of prostate field cancerization. Expression of MIC-1 and PDGF-A was measured quantitatively by immunofluorescence and comprehensively analyzed using two methods of signal capture and several groupings of data generated in human cancerous (n = 25), histologically normal adjacent (n = 22), and disease-free (n = 6) prostate tissues. A total of 208 digitized images were analyzed. MIC-1 and PDGF-A expression in tumor tissues were elevated 7.1x to 23.4x and 1.7x to 3.7x compared to disease-free tissues, respectively (p<0.0001 to p = 0.08 and p<0.01 to p = 0.23, respectively). In support of field cancerization, MIC-1 and PDGF-A expression in adjacent tissues were elevated 7.4x to 38.4x and 1.4x to 2.7x, respectively (p<0.0001 to p<0.05 and p<0.05 to p = 0.51, respectively). Also, MIC-1 and PDGF-A expression were similar in tumor and adjacent tissues (0.3x to 1.0x; p<0.001 to p = 0.98 for MIC-1; 0.9x to 2.6x; p<0.01 to p = 1.00 for PDGF-A). All analyses indicated a high level of inter- and intra-tissue heterogeneity across all types of tissues (mean coefficient of variation of 86.0%). Our data shows that MIC-1 and PDGF-A expression is elevated in both prostate tumors and structurally intact adjacent tissues when compared to disease-free specimens, defining field cancerization. These secreted factors could promote tumorigenesis in histologically normal tissues and lead to tumor multifocality. Among several clinical applications, they could also be exploited as indicators of disease in false negative biopsies, identify areas of repeat biopsy, and add molecular information to surgical margins.

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“…Two representative regions of interest (defined as areas with robust immunostaining,~100 μm 2 each) per slide were chosen, and the cumulative florescence intensity specific for Dyligh 488 (green) was determined. 52 Animal model/immunohistochemical reactions The LLC cells were transplanted into C57BL/6 mice by tail vein injection. The animals were then killed on day 20 after LLC transplantation, and the LLC cells in the lungs were isolated by mincing, collagenase type I digestion and filtering.…”

Section: Immunofluorescencementioning

confidence: 99%

Angiomotin decreases lung cancer progression by sequestering oncogenic YAP/TAZ and decreasing Cyr61 expression

Hsu

et al. 2014

Oncogene

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Lung cancer is the leading cause of cancer death worldwide, with metastasis underlying majority of related deaths. Angiomotin (AMOT), a scaffold protein, has been shown to interact with oncogenic Yes-associated protein/transcriptional co-activator with a PDZ-binding motif (YAP/TAZ) proteins, suggesting a potential role in tumor progression. However, the functional role of AMOT in lung cancer remains unknown. This study aimed to identify the patho-physiological characteristics of AMOT in lung cancer progression. Results revealed that AMOT expression was significantly decreased in clinical lung cancer specimens. Knockdown of AMOT in a low metastatic CL1-0 lung cancer cell line initiated cancer proliferation, migration, invasion and epithelial-mesenchymal transition. The trigger of cancer progression caused by AMOT loss was transduced by decreased cytoplasmic sequestration and increased nuclear translocation of oncogenic co-activators YAP/TAZ, leading to increased expression of the growth factor, Cyr61. Tumor promotion by AMOT knockdown was reversed when YAP/TAZ or Cyr61 was absent. Further, AMOT knockdown increased the growth and spread of Lewis lung carcinoma in vivo. These findings suggest that AMOT is a crucial suppressor of lung cancer metastasis and highlight its critical role as a tumor suppressor and its potential as a prognostic biomarker and therapeutic target for lung cancer.

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Early growth response 1 and fatty acid synthase expression is altered in tumor adjacent prostate tissue and indicates field cancerization

Cited by 14 publications

References 36 publications

Heterogeneous patterns of DNA methylation-based field effects in histologically normal prostate tissue from cancer patients

Heterogeneous patterns of DNA methylation-based field effects in histologically normal prostate tissue from cancer patients

Prostate Field Cancerization: Deregulated Expression of Macrophage Inhibitory Cytokine 1 (MIC-1) and Platelet Derived Growth Factor A (PDGF-A) in Tumor Adjacent Tissue

Angiomotin decreases lung cancer progression by sequestering oncogenic YAP/TAZ and decreasing Cyr61 expression

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